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AT特异性双功能嵌入剂[N-MeCys3,N-MeCys7]TANDEM从DNA的TpA位点解离。

Dissociation of the AT-specific bifunctional intercalator [N-MeCys3,N-MeCys7]TANDEM from TpA sites in DNA.

作者信息

Fletcher M C, Olsen R K, Fox K R

机构信息

Department of Physiology and Pharmacology, Bassett Crescent East, University of Southampton, U.K.

出版信息

Biochem J. 1995 Feb 15;306 ( Pt 1)(Pt 1):15-9. doi: 10.1042/bj3060015.

Abstract

We have examined the dissociation of [N-MeCys3,N-MeCys7]TANDEM, an AT-selective bifunctional intercalator, from TpA sites in mixed-sequence DNAs by a modification of the footprinting technique. Dissociation of complexes between the ligand and radiolabelled DNA fragments was initiated by adding a vast excess of unlabelled calf thymus DNA. Portions of this mixture were subjected to DNAse I footprinting at various times after adding the competitor DNA. Dissociation of the ligand from each site was seen by the time-dependent disappearance of the footprinting pattern. Within a natural DNA fragment (tyrT) the ligand dissociates from TTAT faster than from ATAT. We found that the stability of complexes with isolated TpA steps decreases in the order ATAT > TTAA > TATA. Dissociation from each of these sites is much faster than from longer regions of (AT)n. These results confirm the requirement for A and T base-pairs surrounding the TpA step and suggest that the interaction is strongest with regions of alternating AT, possibly as a result of its unusual structure. The ligand dissociates more slowly from the centre of (AT)n tracts than from the edges, suggesting that variations in dissociation rate arise from sequence-dependent variations in local DNA structure.

摘要

我们通过改进足迹技术,研究了一种AT选择性双功能嵌入剂[N-MeCys3,N-MeCys7]TANDEM从混合序列DNA中TpA位点的解离情况。通过加入大量未标记的小牛胸腺DNA来启动配体与放射性标记DNA片段之间复合物的解离。在加入竞争DNA后的不同时间,对该混合物的部分进行DNA酶I足迹分析。通过足迹模式随时间的消失可以观察到配体从每个位点的解离。在天然DNA片段(tyrT)中,配体从TTAT解离的速度比从ATAT快。我们发现,与孤立的TpA步的复合物稳定性按ATAT > TTAA > TATA的顺序降低。从这些位点中的每一个的解离都比从(AT)n的更长区域快得多。这些结果证实了TpA步周围需要A和T碱基对,并表明与交替AT区域的相互作用最强,这可能是由于其不寻常的结构。配体从(AT)n序列的中心解离比从边缘慢,这表明解离速率的变化源于局部DNA结构的序列依赖性变化。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/aa85/1136475/7e9925a876c6/biochemj00069-0027-a.jpg

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